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DisBind: A database of classified functional binding sites in disordered and structured regions of intrinsically disordered proteins

机译:DisBind:固有紊乱蛋白的无序和结构化区域中分类功能结合位点的数据库

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Background Intrinsically unstructured or disordered proteins function via interacting with other molecules. Annotation of these binding sites is the first step for mapping functional impact of genetic variants in coding regions of human and other genomes, considering that a significant portion of eukaryotic genomes code for intrinsically disordered regions in proteins. Results DisBind (available at http://biophy.dzu.edu.cn/DisBind ) is a collection of experimentally supported binding sites in intrinsically disordered proteins and proteins with both structured and disordered regions. There are a total of 226 IDPs with functional site annotations. These IDPs contain 465 structured regions (ORs) and 428 IDRs according to annotation by DisProt. The database contains a total of 4232 binding residues (from UniProt and PDB structures) in which 2836 residues are in ORs and 1396 in IDRs. These binding sites are classified according to their interacting partners including proteins, RNA, DNA, metal ions and others with 2984, 258, 383, 350, and 262 annotated binding sites, respectively. Each entry contains site-specific annotations (structured regions, intrinsically disordered regions, and functional binding regions) that are experimentally supported according to PDB structures or annotations from UniProt. Conclusion The searchable DisBind provides a reliable data resource for functional classification of intrinsically disordered proteins at the residue level.
机译:背景技术本质上无结构或无序的蛋白质通过与其他分子相互作用而起作用。考虑到真核生物基因组的很大一部分编码蛋白质中固有的无序区域,对这些结合位点的注释是绘制遗传变异在人类和其他基因组编码区域中功能影响的第一步。结果DisBind(可从http://biophy.dzu.edu.cn/DisBind获得)是内在无序的蛋白质以及具有结构化和无序区域的蛋白质中实验支持的结合位点的集合。共有226个具有功能性站点注释的IDP。根据DisProt的注释,这些IDP包含465个结构化区域(OR)和428个IDR。该数据库包含总共4232个结合残基(来自UniProt和PDB结构),其中OR中2836个残基,IDR中1396个残基。这些结合位点根据它们的相互作用伙伴进行分类,包括蛋白质,RNA,DNA,金属离子和其他带有分别带有2984、258、383、350和262注释的结合位点。每个条目都包含特定于站点的注释(结构化区域,内在无序的区域和功能性绑定区域),这些注释根据UniProt的PDB结构或注释在实验上得到支持。结论可搜索的DisBind为在残基水平上对固有无序蛋白的功能分类提供了可靠的数据资源。

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